Rifamycin in Minimal Hepatic Encephalopathy
关键词
抽象
描述
Hepatic encephalopathy (HE) is a highly prevalent neuro-cognitive complication of cirrhosis characterized by cognitive dysfunction, and high rate of subsequent mortality and recurrence. HE also places a tremendous burden with a relentless increase in inpatient stay duration with charges topping $7244.7 million in 20092. There were almost 23,000 hospitalizations for HE in 2009 and far more patients with HE who are being managed as an outpatient in the US. In the NACSELD (North American Consortium for the Study of End-Stage Liver Disease) experience, HE in inpatients is an independent risk factor for mortality and the leading cause of readmissions in patients with cirrhosis.
HE has two major phases, covert or minimal HE (MHE), which is only recognized by specialized tests and overt HE (OHE), which is clinically obvious. OHE forms the tip of the iceberg, while MHE affects as many as 60% of tested patients with cirrhosis.
MHE is associated with changes in specific cognitive domains that result in altered health-related quality of life and daily function. This can promote the development of OHE, impair driving and employment, increase falls and is independently associated with a risk of hospitalizations and mortality.
There is an alteration of gut microbial composition and function (bile acid changes, endotoxemia and gut metabolic products) in cirrhosis, which worsens with disease progression with MHE and OHE. Current treatments for OHE are mostly focused on the gut, including lactulose and rifaximin. However, despite extracting a major toll on disease progression, there is no current guideline to treat MHE. Prior studies using lactulose and rifaximin have been performed in this setting with improvement in brain function, brain MRI changes and microbial function. However, these are still not standard of care.
Rifamycin SV MMX® 200 mg is a gut-specific antibiotic with a long track record of safety that has been FDA approved for the treatment of traveler's diarrhea. Unlike rifaximin, rifamycin-SV MMX mostly affects the colon, where the bacterial load is much larger than in the other parts of the GI tract. The impact of rifamycin on MHE has not been studied to date. This is a randomized double-blind placebo-controlled trial of MHE in patients with cirrhosis.
日期
最后验证: | 01/31/2020 |
首次提交: | 08/21/2019 |
提交的预估入学人数: | 09/04/2019 |
首次发布: | 09/08/2019 |
上次提交的更新: | 02/09/2020 |
最近更新发布: | 02/11/2020 |
实际学习开始日期: | 08/31/2019 |
预计主要完成日期: | 09/14/2020 |
预计完成日期: | 11/14/2020 |
状况或疾病
干预/治疗
Drug: Rifamycin
Other: Placebo
相
手臂组
臂 | 干预/治疗 |
---|---|
Experimental: Rifamycin Rifamycin-SV MMX 600 mg PO two times a day (1200 mg) for 30 days | Drug: Rifamycin Intervention arm |
Placebo Comparator: Placebo Placebo PO two times a day for 30 days | Other: Placebo Placebo arm |
资格标准
有资格学习的年龄 | 18 Years 至 18 Years |
有资格学习的性别 | All |
接受健康志愿者 | 是 |
标准 | Inclusion Criteria: 1. Age 18-75 years 2. Cirrhosis defined by any one of the following 1. Cirrhosis on liver biopsy or transient elastography 2. Nodular liver on imaging 3. Endoscopic or radiological evidence of varices in a patient with chronic liver disease 4. Platelet count <150,000/mm3 and AST/ALT ratio >1 in a patient with chronic liver disease 3. Women of childbearing age will need to be on accepted birth control for 10 days prior to entering study and 30 days after the end of the last dose of the study drug. 4. Cognitive impairment on PHES aggregate score [more than or greater than] -4SD - based on norms published in Allampati et al located at the website www.encephalapp.com17 (This is the accepted diagnosis of minimal HE.) 5. Willing and able to participate, provide samples and complete follow-up 6. Stable Liver function tests between 2-12 weeks prior to enrollment (can include the screening laboratory values details in exclusion criteria) Exclusion Criteria: 1. Unclear diagnosis of cirrhosis (does not meet the criteria outlined above) 2. Child score >8 3. Increasing trend of ALT and AST in the 2-12 weeks prior to study inclusion (Baseline values established by at least two samples obtained at least 2 weeks and no more than 8-12 weeks apart) to account for disease related changes in liver enzymes and bilirubin while on study that may otherwise be inappropriately attributed to study drug. >20% increase in baseline serum AST, ALT, ALP and total bilirubin (TBL) will be considered an exclusion criterion. 4. Unable to consent, follow for the study duration 5. Normal performance on PHES 6. Mini-mental status exam<2518 7. Recent alcohol abuse (within 3 months) 8. Recent illicit drug abuse (within 3 months) except marijuana 9. Current use of psychoactive drugs apart from long-standing opioids or stable anti-depressant use. 10. Prior overt HE episodes defined as West-Haven Criteria grade 2 or higher in the past that required hospitalization or initiation of lactulose or rifaximin therapy 11. Currently on lactulose or rifaximin 12. Current or recent invasive bacterial or fungal infections (<1 month) 13. Allergic reactions to rifamycin, rifampin or rifaximin 14. MELD >20 15. TIPS placement 16. Serum sodium<125 17. On SBP prophylaxis 18. Post-transplant cirrhosis 19. Infections within 4 weeks 20. End-stage organ failures: CHF with EF<25%, End-stage renal disease on dialysis, COPD on home oxygen 21. Pregnancy (positive urine pregnancy test at screening) 22. Current on statin therapy 23. In the opinion of the PI, those who are unlikely to survive or remain without liver transplant for 6 weeks, or cannot adhere to the trial activities. |
结果
主要结果指标
1. Cirrhosis Dysbiosis Ratio of stool microbiota [30 days]
次要成果指标
1. Psychometric hepatic encephalopathy score (PHES) composite score ranges from -15 to +5 [30 days]
2. EncephalApp Stroop OffTime+OnTime is the total time taken to complete 5 runs in Off and 5 runs in On state. [30 days]
3. Sickness Impact Profile total score is the total score determined after all 12 domains are scored [30 days]
4. Sickness Impact Profile psychosocial score is the score of the psychosocial part of the SIP [30 days]
5. Sickness Impact Profile physical score is the score of the physical part of the SIP [30 days]
6. Pittsburgh sleep quality index [30 days]
7. Serious adverse events (Hospitalizations, death, prolongation of hospitalizations) [30 days]
8. Serious adverse events (Hospitalizations, death, prolongation of hospitalizations) [37 days]
9. Adverse events related to rifamycin [30 days]
10. Adverse events related to rifamycin [37 days]
11. Systemic exposure of rifamycin in the blood [Baseline]
12. Systemic exposure of rifamycin in the blood [15 days]
13. Systemic exposure of rifamycin in the urine [Baseline]
14. Systemic exposure of rifamycin in the urine [15 days]
15. Endotoxin levels in serum using LAL assay [30 days]
16. Calprotectin levels in stool [30 days]
17. Serum IL-6 levels [30 days]
18. Serum IL-1beta levels [30 days]
19. Fecal bile acid levels [30 days]
20. Serum bile acid levels [30 days]
21. Microbiota diversity using Shannon index [30 days]
22. Salivary dysbiosis ratio [30 days]
其他成果措施
1. Handgrip strength [30 days]
2. Body Muscle composition [30 days]
3. Brain MR Spectroscopy in Anterior cingulate cortex [30 days]
4. Brain MR Spectroscopy in posterior gray matter [30 days]
5. Brain MR Spectroscopy in right parietal white matter [30 days]